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GWAS 在非洲人群中鉴定到了新的脂质相关位点,并证实了非洲人群内存在异质性关联。

GWAS in Africans identifies novel lipids loci and demonstrates heterogenous association within Africa.

机构信息

Center for Research on Genomics and Global Health, National Human Genome Research Institute, NIH, Bethesda, MD 20892, USA.

出版信息

Hum Mol Genet. 2021 Nov 1;30(22):2205-2214. doi: 10.1093/hmg/ddab174.

Abstract

Serum lipids are biomarkers of cardiometabolic disease risk, and understanding genomic factors contributing to their distribution is of interest. Studies of lipids in Africans are rare, though it is expected that such studies could identify novel loci. We conducted a GWAS of 4317 Africans enrolled from Nigeria, Ghana and Kenya. We evaluated linear mixed models of high-density lipoprotein cholesterol (HDLC), low-density lipoprotein cholesterol (LDLC), total cholesterol (CHOL), triglycerides (TG) and TG/HDLC. Replication was attempted in 9542 African Americans (AA). In our main analysis, we identified 28 novel associations in Africans. Of the 18 of these that could be tested in AA, three associations replicated (GPNMB-TG, ENPP1-TG and SMARCA4-LDLC). Five additional novel loci were discovered upon meta-analysis with AA (rs138282551-TG, PGBD5-HDLC, CD80-TG/HDLC, SLC44A1-CHOL and TLL2-CHOL). Analyses considering only those with predominantly West African ancestry (Nigeria, Ghana and AA) yielded new insights: ORC5-LDLC and chr20:60973327-CHOL. Among our novel findings are some loci with known connections to lipids pathways. For instance, rs147706369 (TLL2) alters a regulatory motif for sterol regulatory element-binding proteins, a family of transcription factors that control the expression of a range of enzymes involved in cholesterol, fatty acid and TG synthesis, and rs115749422 (SMARCA4), an independent association near the known LDLR locus that is rare or absent in populations without African ancestry. These findings demonstrate the utility of conducting genomic analyses in Africans for discovering novel loci and provide some preliminary evidence for caution against treating 'African ancestry' as a monolithic category.

摘要

血清脂质是心血管代谢疾病风险的生物标志物,了解导致其分布的基因组因素很有意义。尽管人们预计此类研究可以确定新的基因座,但对非洲人的脂质研究很少。我们对来自尼日利亚、加纳和肯尼亚的 4317 名非洲人进行了 GWAS 分析。我们评估了高密度脂蛋白胆固醇(HDLC)、低密度脂蛋白胆固醇(LDLC)、总胆固醇(CHOL)、甘油三酯(TG)和 TG/HDLC 的线性混合模型。在 9542 名非裔美国人(AA)中尝试了复制。在我们的主要分析中,我们在非洲人中确定了 28 个新的关联。在可以在 AA 中测试的 18 个中,有 3 个关联得到了复制(GPNMB-TG、ENPP1-TG 和 SMARCA4-LDLC)。在与 AA 的荟萃分析中发现了另外 5 个新的基因座(rs138282551-TG、PGBD5-HDLC、CD80-TG/HDLC、SLC44A1-CHOL 和 TLL2-CHOL)。仅考虑那些主要具有西非血统(尼日利亚、加纳和 AA)的人进行分析产生了新的见解:ORC5-LDLC 和 chr20:60973327-CHOL。在我们的新发现中,有一些基因座与已知的脂质途径有关。例如,rs147706369(TLL2)改变了固醇调节元件结合蛋白的调节基序,该家族的转录因子控制涉及胆固醇、脂肪酸和 TG 合成的一系列酶的表达,rs115749422(SMARCA4)是 LDLR 基因座附近的一个独立关联,在没有非洲血统的人群中很少或不存在。这些发现表明,在非洲人中进行基因组分析以发现新的基因座是有用的,并为谨慎对待“非洲血统”作为一个整体类别提供了一些初步证据。

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